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Increased Nanoparticle Delivery to Brain Tumors by Autocatalytic Priming for Improved Treatment and Imaging

机译:通过自动催化引发增加了纳米颗粒向脑肿瘤的递送,从而改善了治疗和成像

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The blood brain barrier (BBB) is partially disrupted in brain tumors. Despite the gaps in the BBB, there is an inadequate amount of pharmacological agents delivered into the brain. Thus, the low delivery efficiency renders many of these agents ineffective in treating brain cancer. In this report, we proposed an "autocatalytic" approach for increasing the transport of nanoparticles into the brain. In this strategy, a small number of nanoparticles enter into the brain via transcytosis or through the BBB gaps. After penetrating the BBB, the nanoparticles release BBB modulators, which enables more nanoparticles to be transported, creating a positive feedback loop for increased delivery. Specifically, we demonstrated that these autocatalytic brain tumor-targeting poly(amine-co-ester) terpolymer nanoparticles (ABTT NPs) can readily cross the BBB and preferentially accumulate in brain tumors at a concentration of 4.3- and 94.0-fold greater than that in the liver and in brain regions without tumors, respectively. We further demonstrated that ABTT NPs were capable of mediating brain cancer gene therapy and chemotherapy. Our results suggest ABTT NPs can prime the brain to increase the systemic delivery of therapeutics for treating brain malignancies.
机译:血脑屏障(BBB)在脑肿瘤中被部分破坏。尽管血脑屏障之间存在差距,但仍有足够数量的药理药物输送到大脑。因此,低的递送效率使得这些试剂中的许多在治疗脑癌中无效。在此报告中,我们提出了一种“自动催化”方法,用于增加纳米颗粒向大脑的运输。在这种策略中,少数纳米颗粒通过胞吞作用或BBB间隙进入大脑。穿透BBB后,纳米颗粒释放BBB调节剂,从而使更多的纳米颗粒得以运输,从而形成了一个正反馈回路,以增加输送量。具体而言,我们证明了这些靶向脑肿瘤的聚胺-共-酯三元共聚物(ABTT NPs)可以很容易地穿过血脑屏障,并优先在脑肿瘤中蓄积,其浓度比在脑中高4.3-和94.0-倍。肝脏和没有肿瘤的脑区域。我们进一步证明了ABTT NP具有介导脑癌基因治疗和化疗的能力。我们的结果表明,ABTT NP可以引发大脑,从而增加用于治疗脑恶性肿瘤的治疗剂的全身递送。

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